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Tag: kidney disease

  • Kidneycure Grant Applications Now Open
to Support Investigators Committed to Advancing Kidney Health

    Kidneycure Grant Applications Now Open to Support Investigators Committed to Advancing Kidney Health

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    Newswise — Washington, DC (December 1, 2022) —KidneyCure, the grants program supported by the American Society of Nephrology (ASN) Foundation, today announced that applications for its 2023 grants programs are now open. KidneyCure grants support clinical and basic research and kidney health investigators at key professional development milestones. The submission deadline is Wednesday, December 7, 2022, at 2:00 p.m. EST.  Grant applications and guidelines can be found at https://www.kidneycure.org/

    The newly added KidneyCure Diversity, Equity, Inclusion, and Justice Research Scholar Grant, part of the Transition to Independence Grants Program, will fund an ASN member who identifies as underrepresented in medicine or is conducting research focused on diversity, equity, inclusion, or justice.

    More than 37 million Americans suffer from chronic kidney conditions and acute diseases that impact virtually every aspect of their lives as well as their families and communities. Kidney diseases are the ninth leading cause of death in the United States and yet 90% of people with kidney diseases are unaware that they are affected. Dialysis, a therapy for those with kidney failure, has a 5-year mortality rate, which is worse than nearly all forms of cancer and requires billions of dollars annually to manage and treat.

    Investigators funded by KidneyCure are making a difference in key areas that impact kidney health and kidney care for millions of people with kidney diseases. To date, more than 300 grants across its four program categories:   The Pre-Doctoral Fellowship Program fosters early career-stage  PhD students, under the direction of a sponsor, who are highly motivated to make contributions  to the understanding of kidney biology and disease. Grant recipients receive $30,000 per year for up to two years.

    The Ben J. Lipps Fellowship Program helps fellows conduct original, meritorious research projects, conducted under the guidance of a sponsor. This Fellowship serves to establish the beginnings of an independent career and provides $50,000 per year for up to two years.

    The William and Sandra Bennett Clinical Scholars Program supports clinician educators conducting a project that advances all facets of nephrology education and teaching. Recipients are encouraged to complete a formal or educational program during the KidneyCure funded years. Grant recipients receive $50,000 per year for up to two years.

    The newest addition to the program, the KidneyCure Diversity, Equity, Inclusion, and Justice Research Scholar Grant, will fund an ASN member who identifies as underrepresented in medicine or is conducting research focused on diversity, equity, inclusion, or justice. All Transition to Independence Grants provide $100,000 for up to two years to help young faculty become independent researchers.

     

    About KidneyCure

    Established in 2012, KidneyCure funds the Ben J. Lipps Research Fellowship Program, the Transition to Independence Grants Program, the William and Sandra Bennett Clinical Scholars Program, the American Society of Nephrology-Harold Amos Medical Faculty Development Program, and the ASN Pre-Doctoral Fellowship Award Program. For more information, visit www.kidneycure.org, contact [email protected], or call (202) 640-4660.

    About ASN

    Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge and advocating for the highest quality care for patients. ASN has

    more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

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  • Albert Einstein College of Medicine Receives $6.6M in NIH Grants to Lead New York Consortium for Kidney, Urological, and Hematological Research and Training

    Albert Einstein College of Medicine Receives $6.6M in NIH Grants to Lead New York Consortium for Kidney, Urological, and Hematological Research and Training

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    Newswise — November 16, 2022—(BRONX, NY)—The National Institutes of Health has awarded Albert Einstein College of Medicine a five-year, $6.6 million grant to lead a New York-based consortium of medical schools to train young scientists in kidney, urology, and hematology research.

    The grant establishes the New York Consortium for Interdisciplinary Training in Kidney, Urological, and Hematological Research, or NYC Train KUHR (pronounced “cure”), bringing together experts in research and education from Einstein, Columbia University Irving Medical Center, the Icahn School of Medicine at Mount Sinai, and Renaissance School of Medicine at Stony Brook University.

    “With NYC Train KUHR, more than 100 scientists skilled in kidney, urologic, and hematologic (KUH) disease research will work together to mentor pre- and post-doctoral fellows in interdisciplinary research involving these specialties,” said Michal Melamed, M.D., M.S., the grant’s lead principal investigator and professor of medicine, of pediatrics, and of epidemiology & population health at Einstein and a nephrologist at Montefiore Health System. “These specialties are deeply intertwined and it’s critical to train a new generation of investigators who can comfortably navigate these fields and lead research to improve the care and quality of life for people with KUH diseases.”

    “Many of the diseases the trainees will focus on—such as sickle cell disease and kidney disease—disproportionately affect Black and Hispanic people, and other marginalized groups,” continued Dr. Melamed. “We are particularly hopeful that advancing this interdisciplinary training will benefit our Bronx community.”  

    NYC Train KUHR is the only NIH-funded consortium focused on KUH disease research and training in the Northeast and one of only seven nationally. Trainees selected to participate in the program will have at least two mentors, who will help guide and inform their research.

    “Many of the diseases of these three body systems result in complications that impact how the others function, so it’s imperative to reach across disciplines to effectively treat disease,” said co-principal investigator Jonathan Barasch, M.D., professor of medicine, of pathology, and of cell biology at Columbia University Irving Medical Center. “While this program is focused on training early career physicians and scientists, we expect that the participating faculty members will also benefit from increased collaborations across institutions.”

    The new grant builds on decades of established training programs at some of the participating institutions. “Individually, our institutions have impressive track records in basic science, translational, and clinical research achievements within these conditions. Together our strengths are magnified, and we can share our collective expertise with new trainees who will continue to make advances in the field,” said Kirk Campbell, M.D., professor of medicine and co-principal investigator at Icahn School of Medicine at Mount Sinai.

    NYC Train KUHR will recruit up to 10 trainees each year who will have opportunities to work under mentors from various institutions, access data and scientific models from past and current studies, and attend regular networking and professional development presentations.

    The grant also will enable the creation of an undergraduate summer program for students from groups historically underrepresented in medicine who are interested in kidney, urology, or hematology research. “A key priority is enriching the diversity of physicians and researchers in our fields,” said co-principal investigator Sandeep Mallipattu, M.D., chief of the division of nephrology and hypertension at Renaissance School of Medicine at Stony Brook University.

    Other co-principal investigators and project leaders on the grant include Frederick Kaskel, M.D., Ph.D., and Kelvin Davies, Ph.D., at Einstein; Wadie Bahou, M.D., at Renaissance School of Medicine at Stony Brook University; Nancy Green, M.D., at Columbia University Irving Medical Center; and Margaret Baron, M.D., Ph.D., at Icahn School of Medicine at Mount Sinai.

    The grant, titled “New York Consortium for Interdisciplinary Training in Kidney, Urological and Hematological Research (NYC Train KUHR),” was provided by the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK), part of the NIH. (1U2CDK129502 and 1TL1DK136048)

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    About Albert Einstein College of Medicine 
    Albert Einstein College of Medicine is one of the nation’s premier centers for research, medical education and clinical investigation. During the 2022-23 academic year, Einstein is home to 740 M.D. students, 194 Ph.D. students, 118 students in the combined M.D./Ph.D. program, and approximately 225 postdoctoral research fellows. The College of Medicine has more than 1,900 full-time faculty members located on the main campus and at its clinical affiliates. In 2022, Einstein received more than $202 million in awards from the National Institutes of Health. This includes the funding of major research centers at Einstein in cancer, aging, intellectual development disorders, diabetes, clinical and translational research, liver disease, and AIDS. Other areas where the College of Medicine is concentrating its efforts include developmental brain research, neuroscience, cardiac disease, and initiatives to reduce and eliminate ethnic and racial health disparities. Its partnership with Montefiore, the University Hospital and academic medical center for Einstein, advances clinical and translational research to accelerate the pace at which new discoveries become the treatments and therapies that benefit patients. For more information, please visit einsteinmed.edu, follow us on Twitter, Facebook, Instagram, LinkedIn, and view us on YouTube

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  • Study assesses environmental sustainability practices in dialysis facilities

    Study assesses environmental sustainability practices in dialysis facilities

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    Newswise — Highlights

    • Survey results from dialysis facilities in Australia and New Zealand indicate that environmental sustainability is not currently prioritized in facilities’ clinical practice, building design, or infrastructure and management systems.
    • Results highlighted major deficiencies, and thereby opportunities for improvement.

    Washington, DC (November 11, 2022) — Healthcare is a significant contributor to greenhouse gas emissions that impact climate change. In fact, if the global healthcare sector were a country, it would be the fifth-largest emitter on the planet. And within healthcare, dialysis programs contribute disproportionately, with high resource consumption and waste generation. A recent study published in CJASN examined the environmental sustainability practices of dialysis facilities, providing insights into where improvements could be made.

    For the study, Benjamin Talbot, MBBS (The George Institute for Global Health) and his colleagues sent an online survey to the heads of all dialysis facilities in Australia and New Zealand between November 2019 and December 2020. Responses were received from 132 dialysis facilities, representing 33% (122/365) of dialysis services within Australia and New Zealand. Most responses were from public satellite facilities (40%), in-center dialysis facilities (25%) and co-located dialysis and home therapies facilities (21%).

    Opportunities for improvement in environmental sustainability practices were identified in 3 domains:

    • Culture—A minority of facilities reported having an environmental sustainability strategy in place (33%) or undertaking sustainability audits (20%). Only 7% reported the inclusion of environmental training in staff induction programs.
    • Building design, infrastructure, energy use—Few facilities reported using renewable energy (14%), reclaiming reverse osmosis reject water (13%), or motion-sensor light-switches (44%).
    • Operations—A minority of facilities reported having waste management education (36%), auditing waste generation (17%), or considering environmental sustainability in procurement decisions (25%).

    “We have established a baseline of environmental sustainability practices in dialysis facilities in Australia and New Zealand, however, only 33% of dialysis facilities responded to the survey, which suggests that environmental sustainability is not a priority for most dialysis facilities. The responses to the survey regarding dialysis practices confirmed this further and demonstrate numerous areas where improvements can be made,” said Dr. Talbot. “As healthcare professionals, we have a duty to advocate for our patients and protect our planet. Dialysis is a life-saving treatment but it has a huge environmental cost, and we must all work together to find ways to reduce its impact.” 

    Additional study authors include Katherine Barraclough, MBBS, PhD, Matthew Sypek, MBBS, PhD, FRACP, Pedro Gois, MD, PhD, FRACP, FASN, Leila Arnold, MbChB, FRACP, Stephen McDonald, MBBS(Hons), PhD, FRACP, and John Knight, MBBS, MA, MBA, FRACP, FASN, GAICD.

    Disclosures: B Talbot and J Knight are employees of Ellen Medical Devices developing the Affordable Dialysis program. K Barraclough has received research funding from Fresenius Medical Care. P Gois has received consultancy and honoraria fees from Alexion Pharmaceuticals. S McDonald has received research funding from Baxter Healthcare and Astellas Pharmaceuticals and has had advisory or leadership roles with Fresenius Kidney Care Australia. L Arnold reports employment and ownership interest in M and M Renal Limited.

    The article, titled “A Survey of Environmental Sustainability Practices in Dialysis Facilities in Australia and New Zealand,” will appear online at http://cjasn.asnjournals.org/ on November 11, 2022, doi: 10.2215/CJN.08090722.

    The content of this article does not reflect the views or opinions of The American Society of Nephrology (ASN). Responsibility for the information and views expressed therein lies entirely with the author(s). ASN does not offer medical advice. All content in ASN publications is for informational purposes only, and is not intended to cover all possible uses, directions, precautions, drug interactions, or adverse effects. This content should not be used during a medical emergency or for the diagnosis or treatment of any medical condition. Please consult your doctor or other qualified health care provider if you have any questions about a medical condition, or before taking any drug, changing your diet or commencing or discontinuing any course of treatment. Do not ignore or delay obtaining professional medical advice because of information accessed through ASN. Call 911 or your doctor for all medical emergencies.

    About ASN Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on FacebookTwitterLinkedIn, and Instagram.

      

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  • Michelle A. Josephson, MD, FASN, to Become Next President of the American Society of Nephrology

    Michelle A. Josephson, MD, FASN, to Become Next President of the American Society of Nephrology

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    Newswise — Washington, DC (November 6, 2022) — The American Society of Nephrology (ASN) is pleased to announce that Michelle A. Josephson, MD, FASN, will become the society’s next president. Dr. Josephson, who succeeds Susan E. Quaggin, MD, FASN, will assume her new role on January 1, 2023.

    A highly experienced physician and academic leader, Dr. Josephson is currently a professor of Medicine and Surgery at the University of Chicago, medical director of the University of Chicago Kidney and Pancreas Transplant Program, and program director of the Transplant Nephrology Fellowship.

    Dr. Josephson is deeply committed to research, education, and care in the realm of kidney transplantation, with particular interests in living kidney donation, post-transplant bone disease, BK virus, and pregnancy in transplant recipients. Having authored more than 100 articles and 5 book chapters and having presented numerous invited lectures nationally and internationally, Dr. Josephson has helped to shape the field of nephrology—from clinical research to clinical care, to education for the next generation of nephrologists.

    Dr. Josephson currently serves on the ASN Council as President-Elect. She has served as chair of the Transplant Advisory Group, the Policy and Advocacy Committee, and the ASN Early Program on Kidney Transplantation. She has also been a member of numerous ASN committees and groups, including the ASN COVID response team. Dr. Josephson chaired the American Society of Transplantation (AST) Cutting Edge of Transplantation 2020 and 2021 meetings, and the KDIGO Controversies Conference on the Failing Allograft. From 2007 to 2010 she served as a Councilor-at-Large on the AST Board of Directors. From 2005-2006 she was President of Women in Nephrology. She serves on the editorial board of CJASN and was an Associate Editor for Transplantation.

    “It’s an exciting time to be ASN’s incoming president,” said Dr. Josephson. “I’m truly honored to be in this role as we continue to see numerous advances and increased awareness related to kidney health with ASN at the forefront.”

    ASN Kidney Week 2022, the largest nephrology meeting of its kind, will provide a forum for nephrologists and other kidney health professionals to discuss the latest findings in research and engage in educational sessions related to advances in the care of patients with kidney diseases and related disorders.

    Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

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  • Did having kidney disease and other conditions affect COVID-19 outcomes in different waves of the pandemic?

    Did having kidney disease and other conditions affect COVID-19 outcomes in different waves of the pandemic?

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    Highlights

    • During 4 waves of the COVID-19 pandemic in New York City, the risk of severe COVID-19 was associated with pre-existing chronic kidney disease, as well as heart disease, diabetes, and hypertension.
    • The risk of acute kidney injury after developing COVID-19 was also associated with various pre-existing medical conditions.
    • Results from the study will be presented at ASN Kidney Week 2022 November 3–November 6.

    Newswise — Orlando (November 5, 2022) — Individuals with chronic kidney disease (CKD) are vulnerable to developing severe forms of COVID-19, and acute kidney injury is a common complication of COVID-19. A recent analysis examined the temporal effects of pre-existing CKD and other medical conditions on COVID-19 outcomes by waves throughout the pandemic. The findings will be presented at ASN Kidney Week 2022 November 3–November 6. 

    Investigators identified 64,246 COVID-19 cases during 4 waves at Columbia University Medical Center in New York City, with 8% being severe and 18% requiring hospitalization. Among the major findings:

    • The risk of severe COVID-19 was associated with pre-existing CKD, heart disease, diabetes, and hypertension in most waves; and lung disease, obesity, and cancer in at least one wave.
    • Acute kidney injury occurred in 49% of severe cases and 35% of hospitalized ones.
    • The risk of acute kidney injury was associated with heart failure, obesity, diabetes, and cancer in most waves; and CKD, coronary artery disease, hypertension, and stroke in one or two waves.

    “Pre-existing CKD was one of the most consistent clinical predictors of COVID-19 severity, complications, and poor outcomes across multiple pandemic waves,” said lead author Ning Shang, PhD. “Hospitals could include kidney function evaluation in patient populations as part of consideration for planning treatments and evaluating hospital capacities during future pandemic waves” added co-author Krzysztof Kiryluk, MD.

    Study: “Kidney Disease and COVID-19 Outcomes in the Temporal Analysis of Pandemic Waves”

    ASN Kidney Week 2022, the largest nephrology meeting of its kind, will provide a forum for nephrologists and other kidney health professionals to discuss the latest findings in research and engage in educational sessions related to advances in the care of patients with kidney diseases and related disorders.

    Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

     

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  • The COVID-19 pandemic has had direct and indirect impacts on the mortality of patients on dialysis

    The COVID-19 pandemic has had direct and indirect impacts on the mortality of patients on dialysis

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    Highlights

    • During the COVID-19 pandemic in 2020, mortality risk for both COVID-19–positive and other patients on hemodialysis fluctuated in line with two waves of the pandemic in the general population.
    • Compared with hemodialysis patients treated in 2019, the mortality risk of COVID-19–positive patients on dialysis persisted at much higher levels across 2020, whereas the mortality risk of other patients on dialysis was elevated slightly and mainly during the pandemic peak period.
    • Results from the study will be presented at ASN Kidney Week 2022 November 3–November 6.

    Newswise — Orlando (November 5, 2022) — New research has revealed elevated risks of death during the COVID-19 pandemic for both COVID-19–positive and other patients on hemodialysis compared with hemodialysis patients treated in 2019. The findings will be presented at ASN Kidney Week 2022 November 3–November 6.

    The study relied on data from 63,216 patients undergoing hemodialysis in 2019–2020 at NephroCare centers of 23 countries in European and Middle East countries.

    In line with two waves of the pandemic in the general population, two fluctuations of mortality risk were observed for both COVID-19–positive and other patients on hemodialysis (patients without a documented COVID-19 infection in Fresenius Medical Care’s electronic health record system). Compared with hemodialysis patients treated in 2019, the mortality risk of COVID-19–positive patients on dialysis persisted at much higher levels across 2020 (greater than 6.5-fold), whereas the mortality risk of other patients on dialysis was elevated slightly (less than 1.5-fold) and mainly during the pandemic peak periods.

    “The COVID-19 pandemic had direct and indirect impact on the mortality of hemodialysis patients,” said corresponding author Yan Zhang, PhD, of Fresenius Medical Care. “Potential reasons of the increased mortality among patients without confirmed COVID-19 diagnosis could be undertesting or healthcare system capacity constraints. Quantifying the magnitude of pandemic effects on patients with and without confirmed disease may benefit dialysis clinics to manage patients during critical events.” 

    Study: “COVID-19 pandemic effect on mortality of hemodialysis patients”

    ASN Kidney Week 2022, the largest nephrology meeting of its kind, will provide a forum for nephrologists and other kidney health professionals to discuss the latest findings in research and engage in educational sessions related to advances in the care of patients with kidney diseases and related disorders.

    Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

     

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  • Strategy Suggests Combining Surrogate Markers for Kidney Disease Progression in Clinical Trials

    Strategy Suggests Combining Surrogate Markers for Kidney Disease Progression in Clinical Trials

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    Highlights

    • In clinical trials of patients with chronic kidney disease, combining information from the treatment effects on two markers of kidney disease progression—urinary albumin:creatinine ratio change and glomerular filtration rate slope—improves predictions of treatment effects on clinical endpoints.
    • Results from the study will be presented at ASN Kidney Week 2022 November 3–November 6.

    Newswise — Orlando (November 5, 2022) — Change in urinary albumin:creatinine ratio (UACR) and glomerular filtration rate (GFR) slope are markers that are individually used as surrogates of chronic kidney disease progression in clinical trials. Investigators recently developed a strategy that combines information from the treatment effects on the two to improve the prediction of treatments’ effects on patient outcomes. Their research will be presented at ASN Kidney Week 2022 November 3–November 6.

    The scientists used data from 41 randomized controlled trials of chronic kidney disease progression to develop their strategy and then applied the results to the design of a phase 2 trial to assess design implications (such as sample size and follow-up time) for using UACR change and GFR slope individually or in combination.

    The analysis revealed that in phase 2 clinical trials with sample sizes of 100–200 patients per arm or follow-up times ranging between 1 and 2 years, combining UACR change and GFR slope improves predictions of treatments’ effects on clinical endpoints.

    “Currently, UACR change and GFR slope are often evaluated as separate endpoints in phase 2 trials; however, it is not clear how to integrate the information provided by these two endpoints,” said corresponding author Tom Greene, PhD, of the University of Utah. “This work presents a 2-step methodology for addressing this problem. In the first step, a Bayesian model is used to characterize the relationships among the treatment effects on UACR, GFR slope, and the clinical endpoint across previous randomized trials. In the second step, this model is used to provide a unified estimate of the probability of clinical benefit based on the estimated effects of the treatment on UACR change and GFR slope in a new phase 2 trial.”

    Study: “Change in albuminuria and GFR slope as joint surrogate endpoints for kidney failure – Implications for phase 2 trials”

    ASN Kidney Week 2022, the largest nephrology meeting of its kind, will provide a forum for nephrologists and other kidney health professionals to discuss the latest findings in research and engage in educational sessions related to advances in the care of patients with kidney diseases and related disorders.

    Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

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  • Conservative management vs. dialysis for preventing hospitalizations in patients with advanced kidney diseases and different ethnicities

    Conservative management vs. dialysis for preventing hospitalizations in patients with advanced kidney diseases and different ethnicities

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    Highlights

    • Researchers have compared the impact of conservative management vs. dialysis on hospitalization outcomes in patients with advanced kidney disease across different races/ethnicities.
    • Results from the study will be presented at ASN Kidney Week 2022 November 3–November 6.

    Newswise — Orlando (November 5, 2022) — For some individuals with advanced kidney disease, dialysis may not be the optimal treatment strategy for their condition, and these patients may be better served with conservative non-dialytic management that focuses on quality of life and symptom control. Investigators recently examined the differential impact of conservative management vs. dialysis on hospitalization outcomes across varying racial/ethnic groups in a large national cohort of patients with advanced kidney disease. The research will be presented at ASN Kidney Week 2022 November 3–November 6. 

    In this study, the investigators compared hospitalization rates among 309,188 patients with advanced kidney disease who were treated with conservative management or dialysis over the period of 2007–2020. During follow-up, 55% of patients had 1 or more hospitalizations, and the most common causes of hospitalization in both groups were related to congestive heart failure/fluid overload, respiratory problems, or hypertension.

    In Non-Hispanic White, Non-Hispanic Black, and Hispanic patients, patients on dialysis had higher hospitalization rates than those who received conservative management, and patients who started dialysis early (transitioned to dialysis at higher levels of kidney function) demonstrated the highest rates across all age groups when compared with those who started dialysis late (transitioned to dialysis at lower levels of kidney function) or were treated with conservative management. Among Asian patients, those on dialysis also had higher hospitalization rates than those receiving conservative management, but patients who started dialysis late had higher rates than those on early dialysis, especially in older age groups.


    “There has been growing recognition of the importance of conservative non-dialytic management as an alternative patient-centered treatment strategy for advanced kidney disease. However, conservative management remains under-utilized in the US, which may in part be due to uncertainties regarding which patients will most benefit from dialysis vs. non-dialytic treatment,” said corresponding author Connie Rhee, MD, of the University of California, Irvine. “We hope that these findings and further research can help inform treatment options for patients, care partners, and providers in the shared decision-making process of conservative management vs. dialysis.”

     Study: “Impact of Race/Ethnicity and Age on Hospitalization Outcomes in Advanced CKD Patients Treated with Conservative Management vs. Dialysis”

    ASN Kidney Week 2022, the largest nephrology meeting of its kind, will provide a forum for nephrologists and other kidney health professionals to discuss the latest findings in research and engage in educational sessions related to advances in the care of patients with kidney diseases and related disorders.

    Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

     

     

     

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  • Risks of kidney failure and death differ in Black and white veterans over time after chronic kidney disease onset

    Risks of kidney failure and death differ in Black and white veterans over time after chronic kidney disease onset

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    Highlights

    • Among US veterans with chronic kidney disease (CKD), Black individuals had a higher risk of developing kidney failure compared with White veterans, and their risk was more pronounced in the early years after kidney disease onset.
    • The overall risk of death was similar in Black and White veterans, but Blacks had a higher risk early on, followed by a lower risk thereafter.
    • Results from the study will be presented at ASN Kidney Week 2022 November 3–November 6.

    Newswise — Orlando (November 4, 2022) — In an analysis of data on US veterans with chronic kidney disease (CKD), risks of kidney failure and death varied for Black compared with White veterans over time, with Black individuals being especially vulnerable in the early years after developing CKD. The research will be presented at ASN Kidney Week 2022 November 3–November 6.

    The study included 180,881 White and 32,187 Black veterans who developed CKD from 2003–2008 and were followed through 2018.

    During follow-up, the adjusted risk of kidney failure was 30% greater in Blacks than in Whites, but this difference was more pronounced over the early years of CKD onset (for example, a 38% greater risk in years 0–2) than at later years (only 8% greater risk in years 8–10). Despite an overall similar mortality risk after adjusting for major confounding factors, there was a greater risk of death for Blacks during the first 4 years of CKD onset, followed by a lower risk thereafter.

    These risk differences over time were consistent across subgroups, such as those with and without comorbidities including hypertension, diabetes, and cardiovascular diseases.

    “Black adults are particularly susceptible to kidney failure and death during the first several years of CKD onset. This result demands a stronger urgency for close evaluation in the earlier years of CKD to improve outcomes,” said corresponding author Guofen Yan, PhD, of the University of Virginia.

    Study: “Time-dependent risk differences in kidney failure and death between Black and White veterans following incident CKD”

    ASN Kidney Week 2022, the largest nephrology meeting of its kind, will provide a forum for nephrologists and other kidney health professionals to discuss the latest findings in research and engage in educational sessions related to advances in the care of patients with kidney diseases and related disorders.

    Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

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  • Long-Term Exposure to Air Pollution May Increase Kidney Disease Risk

    Long-Term Exposure to Air Pollution May Increase Kidney Disease Risk

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    Highlights

    • Among adults with normal kidney function, exposure to higher concentrations of components of air pollution was linked with higher risks of later developing chronic kidney disease.
    • Compared with individuals with high genetic risk of developing kidney disease, those with high air pollution exposure and low genetic risk faced a higher risk of developing chronic kidney disease.  
    • Results from the study will be presented at ASN Kidney Week 2022 November 3–November 6.

    Newswise — Orlando (November 4, 2022) — Both genetic and environmental factors contribute to chronic kidney disease (CKD). New research assessed the interaction of air pollution and genetic factors on the development of CKD. The research will be presented at ASN Kidney Week 2022 November 3–November 6. 

    Investigators analyzed data from 350,994 participants without CKD at baseline in the UK Biobank. Exposure to higher concentrations of components of air pollution was linked with higher risks of developing CKD. Compared with individuals with high genetic risk of developing CKD, those with high air pollution exposure and low genetic risk faced a higher risk of developing CKD. 

    “Long-term exposure to air pollution may increase the risk of CKD, especially in those with low genetic risk,” the authors wrote.

    Study: “Air pollution, genetic factors, and the risk of incident chronic kidney disease: a prospective study of polygenic risk score analysis in the UK Biobank”

    ASN Kidney Week 2022, the largest nephrology meeting of its kind, will provide a forum for nephrologists and other kidney health professionals to discuss the latest findings in research and engage in educational sessions related to advances in the care of patients with kidney diseases and related disorders.

    Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

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    American Society of Nephrology (ASN)

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  • New Onset Chronic Kidney Disease in People with Diabetes Highest Among Ethnic, Racial Minorities

    New Onset Chronic Kidney Disease in People with Diabetes Highest Among Ethnic, Racial Minorities

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    Newswise — New onset chronic kidney disease (CKD) in people with diabetes is highest among racial and ethnic minority groups compared with white persons, a UCLA-Providence study finds.

    The study, published as a letter to the editor in the New England Journal of Medicine, found that new onset CKD rates were higher by approximately 60%, 40%, 33%, and 25% in the Native Hawaiian/Pacific Islander, Black, American Indian/Alaska Native, and Hispanic/Latino populations, respectively, compared to white persons with diabetes.

    Although high CKD incidence in diabetes persists, the rate declined from 8% of the overall diabetes population in 2015-2016 to 6.4% in 2019-2020”.

    “The results of our study constitute a call to action to institute directed, targeted efforts aimed at deliberately shifting the trajectory of persistently high rates of diabetes-related CKD and kidney failure that disproportionately affect racial and ethnic minority groups,” said co-author Dr. Susanne Nicholas, associate professor of medicine in the division of nephrology at the David Geffen School of Medicine at UCLA and chair of the UCLA Nephrology Racial and Health Equity Committee. “The first step should be to increase the rates of screening and detection of CKD in individuals with diabetes.”

    Researchers from the Geffen School, Providence, and the Centers for Disease Control and Prevention tracked 654,549 adults with diabetes from 2015 through 2020 using electronic health records from Providence Health and UCLA Health, two large not-for-profit health systems serving the Western United States.

    The prevalence of kidney failure requiring dialysis or transplant more than doubled to nearly 800,000 persons in the United States between 2000 and 2019, with diabetes as the leading cause. The rate of new onset of CKD in people with diabetes was previously unknown, yet the value of such incidence data is vital for identifying high-risk populations, determining the effectiveness of interventions, and assessing the effects on health care delivery and public health responses. Even more striking, less than 10% of patients with early stage kidney disease are aware of having CKD at this stage in its progression, when therapies are most effective. 

    “Given the rapidly growing population with diabetes in the United States and the corresponding high rates of kidney failure, the persistently high incidence of CKD marked by racial and ethnic disparities is troubling,” said lead author Dr.  Katherine Tuttle, executive director for research at Providence Inland Northwest Health and professor of medicine at the University of Washington. “Inclusive strategies for prevention, detection, and intervention are needed to reduce CKD risk in people with diabetes.”

    Additional study authors are Dr. O. Kenrik Duru and Dr. Keith Norris of UCLA; Cami Jones, Kenn Daratha, Dr. Radica Alicic, and Joshua Neumiller of Providence; and Nilka Ríos Burrows, Alain Koyama, and Dr. Meda Pavkov of the Centers for Disease Control and Prevention.

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    University of California, Los Angeles (UCLA), Health Sciences

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  • Study assesses symptom trajectories and outcomes in patients with kidney disease

    Study assesses symptom trajectories and outcomes in patients with kidney disease

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    Highlights

    • Among individuals with varying levels of chronic kidney disease who were not on dialysis, the prevalence of individual symptoms ranged from 24% (chest pain) to 83% (fatigue), and 98% of participants reported at least one symptom.
    • Patients categorized as having a “Worse symptom score and worsening trajectory” of symptoms had higher risks of later needing dialysis and of dying before dialysis initiation.

    Newswise — Washington, DC (October 28, 2022) — When individuals with varying degrees of chronic kidney disease who were not on dialysis answered annual questionnaires about their symptoms, researchers found that one-third could be categorized as having a “Worse symptom score and worsening trajectory” of symptoms. As reported in CJASN, these patients had especially high risks of later needing dialysis and of dying before dialysis initiation.

    For the study, Moustapha Faye, MD (CHRU Nancy, Université Cheikh Anta Diop de Dakar) and his colleagues, investigators of the CKD-REIN cohort study, assessed symptoms annually using the Kidney Disease Quality of Life-36 questionnaire that was completed by 2,787 adults in France with CKD who were not on dialysis.

    The prevalence of each symptom ranged from 24% (chest pain) to 83% (fatigue), and 98% of participants reported at least one symptom. After a median follow-up of 5.3 years, 690 participants initiated kidney replacement therapy (KRT) such as dialysis, and 490 died before KRT. The team identified two profiles of symptom trajectories: a “Worse symptom score and worsening trajectory” in 31% of participants, characterized by a low initial symptom score that worsened more than 10 points (on a scale of 0–100) over time, and a “Better symptom score and stable trajectory” in 69% of participants, characterized by a high initial score that remained stable over time.

    Participants in the “Worse symptom score and worsening trajectory” category had more risk factors for CKD progression at baseline, worse quality of life, and a higher risk of KRT and death before KRT than other participants.

    “In addition to the already existing classifications of CKD, it is possible to actively monitor symptoms and classify patients according to their progression. This monitoring should involve practitioners and patients,” said Dr. Faye. “This active symptom tracking will allow early therapeutic interventions to be planned to help manage different symptoms.”

    An accompanying editorial notes that “in addition to disease management, Faye et al. provide further evidence of the need to care for the unpleasant symptoms that cause suffering and affect the well-being of patients with advanced CKD”

    Additional study authors include Karine Legrand, PhD; Lisa Le Gall; Karen Leffondre, PhD; Abdou Y. Omorou, MD, PhD; Natalia Alencar de Pinho, PhD; Christian Combe, MD, PhD; Denis Fouque, MD, PhD; Christian Jacquelinet, PhD; Maurice Laville, PhD; Sophie Liabeuf, PhD; Ziad A Massy, MD, PhD; Elodie Speyer, PhD; Roberto Pecoits Filho, PhD; Bénédicte Stengel, MD, PhD; Luc Frimat, MD, PhD; and Carole Ayav, MD; and the CKD-REIN Study Group.

    Disclosures: The authors reported no financial disclosures.

    The article, titled “Five-Year Symptom Trajectories in Non-Dialysis Dependent Chronic Kidney Disease Patients,” will appear online at http://cjasn.asnjournals.org/ on October 28, 2022, doi: 10.2215/CJN.06140522.

    The editorial, titled “Can We Turn the Symptom Curve? Symptom Trajectories and Outcomes among Patients with CKD,” will appear online at http://cjasn.asnjournals.org/ on October 28, 2022, doi: 10.2215/CJN.11240922. 

    The content of this article does not reflect the views or opinions of The American Society of Nephrology (ASN). Responsibility for the information and views expressed therein lies entirely with the author(s). ASN does not offer medical advice. All content in ASN publications is for informational purposes only, and is not intended to cover all possible uses, directions, precautions, drug interactions, or adverse effects. This content should not be used during a medical emergency or for the diagnosis or treatment of any medical condition. Please consult your doctor or other qualified health care provider if you have any questions about a medical condition, or before taking any drug, changing your diet or commencing or discontinuing any course of treatment. Do not ignore or delay obtaining professional medical advice because of information accessed through ASN. Call 911 or your doctor for all medical emergencies.

    About ASN Since 1966, ASN has been leading the fight to prevent, treat, and cure kidney diseases throughout the world by educating health professionals and scientists, advancing research and innovation, communicating new knowledge, and advocating for the highest quality care for patients. ASN has more than 20,000 members representing 132 countries. For more information, visit www.asn-online.org and follow us on Facebook, Twitter, LinkedIn, and Instagram.

     

     

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    American Society of Nephrology (ASN)

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  • Alcoholic Pancreatitis Patients with Continued Alcohol Intake May Finally Have Therapeutic Options

    Alcoholic Pancreatitis Patients with Continued Alcohol Intake May Finally Have Therapeutic Options

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    Newswise — Many alcoholic pancreatitis patients continued drinking during COVID-19. University of Miami Miller School of Medicine researchers study the effects of continued alcohol intake and seek better treatment for alcohol-associated pancreatic disease.

    Researchers at the Miller School are looking for solutions to the continued effects of alcohol use, its harmful impact, and treatment. Understanding the mechanisms of alcohol abuse has gained importance, especially after the COVID-19 pandemic. Higher alcohol consumption led to an increased burden of pancreatic diseases in society.

    In a study titled “Urolithin A attenuates severity of chronic pancreatitis associated with continued alcohol intake by inhibiting PI3K/AKT/mTOR signaling,” published in the American Journal of Physiology – Gastrointestinal and Liver Physiology, researchers examine the short- and long-term consequences of this increased alcohol effect on pancreatic diseases and work together on innovative approaches to better understand how to treat pancreatitis patients with continued alcohol intake.

    Pancreatitis is inflammation of the pancreas often associated with long-term alcohol consumption, a potential risk factor for the induction of acute pancreatitis. Recurrent attacks of acute pancreatitis results in chronic pancreatitis. Each year, about 275,000 hospital stays for acute pancreatitis and 86,000 hospital stays for chronic pancreatitis occur across the U.S., according to the statistics released by the National Institute of Diabetes and Digestive and Kidney Diseases.

    Acute pancreatitis appears suddenly and can typically be resolved in days with treatment in most patients. However, acute pancreatitis can also cause severe life-threatening conditions in some cases. Recurrent episodes of acute pancreatitis instigate irreversible damage to the pancreas, causing weight loss, pain, diabetes, and even pancreatic cancer.

    Alcohol Use Spiked during COVID-19

    Total alcohol sales almost tripled in the U.S. during the COVID-19 pandemic, subsequently increasing the number of patients diagnosed with alcohol-associated pancreatitis. Excessive alcohol consumption is associated with 40-70% of pancreatitis cases. Without moderation, alcohol use harshly impacts both the liver and pancreas, causing fat accumulation and inflammation, disrupting normal function.

    With repeated episodes of binge drinking (four to five drinks in two hours), the pancreas eventually builds up scar tissues with persistent inflammation, weakening its endocrine and exocrine functions needed to digest food and regulate blood sugar levels. This chronic insult to the organ can cause excruciating pain, malnutrition, diabetes, and death.

    “We are developing novel models to study and to prevent inflammation or reverse the pancreatic damage caused due to excess alcohol intake,” said lead author Nagaraj Nagathihalli, Ph.D., associate professor of surgery in the DeWitt Daughtry Family Department of Surgery, Division of Surgical Oncology.

    Continued Alcohol Use Perpetuates Pancreatic Injury in Mice Models

    Accumulating scientific evidence suggests that continued alcohol consumption with established alcoholic pancreatitis instigates irreversible pancreatic damage due to recurrent episodes of acute pancreatitis by fostering a continuous fibro-inflammatory microenvironment within the pancreas.

    “The molecular mechanisms involved in the pathophysiology of alcoholic pancreatitis with continuous alcohol intake remains ambiguous; treatment options and preventative care strategies are restricted due to limited experimental animal models that successfully recapitulate human pancreatitis arising from prolonged or continued alcohol use after established pancreatic injury,” said Dr. Nagathihalli.

    “In this study, using an established alcoholic pancreatitis mice model, we have addressed two of the major unanswered questions with regards to the pathogenesis of pancreatitis. We’ve characterized the pancreas-specific signaling pathways in this process and determined if utilizing novel therapeutic agents can attenuate the severity of alcoholic pancreatitis progression, despite continued alcohol triggers” said first author of the study Siddharth Mehra, Ph.D., a postdoctoral fellow in the Miller School’s Department of Surgery.

    Preventing Alcohol-associated Chronic Pancreatitis May Benefit Patients with Difficulty in Alcohol Abstinence

    The microbiome has been implicated in gastrointestinal inflammation as a critical mediator of overall gut health. Urolithin A is a natural compound synthesized by gut bacteria from ingested ellagitannins, a class of hydrolyzable tannins found mainly in pomegranate, berries, and nuts. Previous work from the group has shown that Urolithin A is a potent anti-inflammatory agent in several pre-clinical disease models and exhibits anti-tumor activity in gastrointestinal cancers.

    “Our studies have demonstrated that Urolithin A is well tolerated and does not elicit any adverse toxic effects at clinically relevant doses in mice. However, despite the promising effect of Urolithin A in several malignancies and inflammatory disorders, the benefit of this microbial metabolite in the prevention of pancreatitis had not been investigated,” says Dr. Nagathihalli. The FDA recognizes Urolithin A as a “safe dietary supplement.”

    “In animal experiments, we have shown that Urolithin A can help improve the effectiveness of treating alcoholic pancreatitis despite continued alcohol intake,” said Dr. Mehra.

    Co-authors of the study include Dr. Chanjuan Shi of Duke University; Dr. Michael VanSaun of the University of Kansas; Dr. Venkatakrishna Jala of the University of Louisville; and Supriya Srinivasan, Ph.D., Samara Singh, Zhiqun Zhou, M.D., Vanessa Garrido, Ph.D., Iago Castro Silva, M.D., Tulasigeri Totiger, Ph.D., Austin Dosch, M.D., Xizi Dai, Ph.D., Rajinder Dawra, Ph.D., Jashodeep Datta, M.D., and Nipun Merchant, M.D., of the Miller School of Medicine.

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    University of Miami Health System, Miller School of Medicine

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  • Lowering the Cost of Insulin Could Be Deadly

    Lowering the Cost of Insulin Could Be Deadly

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    When I heard that my patient was back in the ICU, my heart sank. But I wasn’t surprised. Her paycheck usually runs short at the end of the month, so her insulin does too. As she stretches her supply, her blood sugar climbs. Soon the insatiable thirst and constant urination follow. And once her keto acids build up, her stomach pains and vomiting start. She always manages to make it to the hospital before the damage reaches her brain and heart. But we both worry that someday, she won’t.

    The Inflation Reduction Act, passed last month, aims to help people like her by lowering the cost of insulin across America. Although efforts to expand protections to privately insured Americans were blocked in the Senate, Democrats succeeded in capping expenses for the drug among Americans on Medicare at $35 a month, offering meaningful savings for our seniors, some of whom will save hundreds of dollars a month thanks to the measure. In theory, the policy (and similar ones at the state level) will help the estimated 25 percent of Americans on insulin who have been forced to ration the drug because of cost, and will prevent some of the 600 annual American deaths from diabetic ketoacidosis, the fate from which I’m trying to save my patient.

    Indeed, laws capping co-payments for insulin are welcome news both financially and medically to patients who depend on the drug for survival. However, in their current version, such laws might backfire, leading to even more diabetes-related deaths overall.

    How could that be true? Thanks to the development of new drugs, insulin’s role in diabetes treatment has been declining over the past decade. It remains essential to the small percent of patients with type 1 diabetes, including my patient. But for the 90 percent of Americans with diabetes who have type 2, it should not routinely be the first-, second-, or even third-line treatment. The reasons for this are many: Of all diabetes medications, insulin carries the highest risk of causing dangerously low blood sugar. The medication most commonly comes in injectable form, so administering it usually means painful needle jabs. All of this effort is rewarded with (usually unwanted) weight gain. Foremost and finally, although insulin is excellent at tamping down high blood sugar—the hallmark of diabetes and the driver of some of its complications—it is not as impressive as other medications at mitigating the most deadly and debilitating consequences of the disease: heart attacks, kidney disease, and heart failure.

    Large clinical trials have shown that two newer classes of diabetes medicines, SGLT2 inhibitors and GLP-1 receptor agonists, outperform alternatives (including insulin) in reducing the risk of these disabling or deadly outcomes. Giving patients these drugs instead of older options over a period of three years prevents, on average, one death for about every 100 treated. And SGLT2 inhibitors and GLP-1 receptor agonists pose less risk of causing dangerously low blood sugar, generally do not require frequent injections, and help patients lose weight. Based on these data, the American Diabetes Association now recommends SGLT2 inhibitors and GLP-1 receptor agonists be used before insulin for most patients with type 2 diabetes.

    When a young person dies from diabetic ketoacidosis because they rationed insulin, the culprit is clear. But when a patient with diabetes dies of a heart attack, the absence of an SGLT2 inhibitor or GLP-1 receptor agonist doesn’t get blamed, because other explanations abound: their uncontrolled blood pressure, the cholesterol medication they didn’t take, the cigarettes they continued to smoke, bad genes, bad luck. But every year, more than 1,000 times more Americans die of heart disease than DKA, and of those 700,000 deaths, a good chunk are diabetes-related. (The exact number remains murky.) Diabetes is a major reason that more than half a million Americans depend on dialysis to manage their end-stage kidney disease, and that about 6 million live with congestive heart failure. The data are clear—SGLT2 inhibitors and GLP-1 receptor agonists could help reduce these numbers.

    Still, uptake of these lifesaving drugs is sluggish. Only about one in 10 people with type 2 diabetes is taking them (fewer still among patients who are not wealthy or white). The main cause is simple and stupid: American laws prioritize profits and patents over patients. Because SGLT2 inhibitors and GLP-1 receptor agonists remain under patent protections, drug companies can charge exorbitant rates for them: hundreds if not thousands of dollars a month, sometimes even more than insulin. Doctors spend hours completing arduous paperwork in the hopes of persuading insurers to help our patients, but we’re frequently denied anyway. And even when we do succeed, many patients are left with painful co-payments and deductibles. The most maddening part is that despite their substantial up-front expense, these medications are quite cost-effective in the long run because they prevent pricey complications down the road.

    This is where addressing the cost of insulin—and only insulin—becomes problematic. Doctors are forced daily to decide between the best medication for our patients and the medication that our patients can afford. Katie Shaw, a primary-care physician with a bustling practice at Johns Hopkins, where I’m a senior resident, told me that plenty of her patients can’t afford SGLT2 inhibitors and GLP-1 receptor agonists. In such instances, Shaw is forced to use older oral alternatives and occasionally insulin. “They’re better than nothing at all,” she said.

    If the cost of insulin is capped on its own, insulin will be more likely to jump in front of SGLT2 inhibitors and GLP-1 receptor agonists in treatment plans. That will mean more disease, more disability, and more death from diabetes.

    Medicare patients might avoid some of these effects thanks to provisions in the IRA allowing Medicare to negotiate drug prices and capping out-of-pocket spending on prescriptions at $2,000 a year. The law also guarantees price negotiations for a handful of medications, but SGLT2 inhibitors and GLP-1 receptor agonists won’t necessarily be on the list. And most Americans are not on Medicare. Already, Shaw said, the patients in her practice who tend to be least able to afford SGLT2 inhibitors and GLP-1 receptor agonists are working-class people with private insurance. Some health centers, including the one Shaw and I work at, enjoy access to a federal drug-discount program that can make patent-protected medications, including SGLT2 inhibitors and GLP-1 receptor agonists, more affordable for the uninsured. But most Americans without insurance aren’t so lucky.

    It would be cruel to choose between a world in which more people with type 2 diabetes are nudged toward a drug that won’t stave off the most dangerous complications, and one in which those with type 1 diabetes are priced out of life. In place of capping the out-of-pocket cost of just insulin, lawmakers should cap the out-of-pocket cost of all diabetes medications. This will both protect Americans dependent on insulin and smooth SGLT2 inhibitors’ and GLP-1 receptor agonists’ path to their revolutionary public-health potential.

    The argument for lowering the cost of these drugs for patients is the same as the argument for insulin affordability: that it is both foolish and inhumane to make lifesaving diabetes medications unaffordable when their use prevents costly and deadly downstream complications.

    Patients like mine need affordable access to insulin. But even more need access to SGLT2 inhibitors and GLP-1 receptor agonists. If the laws stop at insulin, many Americans could die unnecessarily—not from inadequate access to insulin, but from preferential access to it.

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    Michael Rose

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